Friday, 24 February 2006

Why are we able to follow a complex conversation while even apes can only understand individual words? German researchers from the Max Planck Institute have used the fMRI (functional magnetic resonance imaging) technique to discover that our brains are hard-wired for grammar. They found that simple language structures are processed by an area of our brain that we share with apes. On the contrary, complex language structures are processed by a 'younger' part or our brains that apes don't have.

s the prism of our senses, the human brain has ways of refracting sensory input in defiance of reality.

This is seen, for example, in the placebo effect, when simple sugar pills or inert salves taken by unwitting subjects are seen to ease pain or have some other beneficial physiological effect. How the brain processes this faked input and prompts the body to respond is largely a mystery of neuroscience.

Now, however, scientists have begun to peel back some of the neurological secrets of this remarkable phenomenon and show how the brain can be rewired in anticipation of sensory input to respond in prescribed ways. Writing in the current issue (March 1, 2006) of the journal Brain, Behavior, and Immunity, a team of University of Wisconsin-Madison scientists reports the results of experiments that portray the brain in action as it is duped.

The new work, conducted by a team led by UW-Madison assistant professor of psychology and psychiatry Jack B. Nitschke, tested the ability of the human brain to mitigate foul taste through a ruse of anticipation. The work, conducted at the UW-Madison Waisman Center using state-of-the-art brain imaging techniques and distasteful concoctions of quinine on a cohort of college students, reveals in detail how the brain responds to a manipulation intended to mitigate an unpleasant experience.

"There is a potent impact to expectancy," says Nitschke, who, with his colleagues, exposed 43 undergraduate subjects to potions of quinine, sugar water or distilled water while undergoing magnetic resonance imaging (MRI).

The subjects, Nitschke explains, were asked beforehand to associate a prescribed set of cues with a taste. A "minus sign" flashed through fiber optic goggles to subjects undergoing MRI, for instance, was to be an anticipatory signal that a liquid subsequently dripped into the mouth would have a very bitter taste. A "zero "cue corresponded with a neutral taste, and a "plus sign" with a pleasant, sugary taste.

The cues, according to Nitschke, were flashed to subjects just prior to the administration of a few drops of liquid. But in the study, the cues would not always match the taste they were said to presage.

His group observed that when subjects were given a cue that suggested the taste they were about to experience would be less bitter, the taste was perceived as such, and the regions of the brain that code tastes were activated less.

"When the subject sees the warning signal, portions of the brain activated by the misleading cue predict the decreased brain response to the awful taste," Nitschke says. What's more, "the (brain's) response to the misleading cue will predict the subject's perception of what the taste is going to be. The subject anticipates that the taste won't be that bad, and indeed that's what they report."

In short, the new study shows how expectancy affects how humans perceive sensory input, and how events in the brain are directly related to those perceptions.

Importantly, by mapping how the brain anticipates an event and kicks in a placebo effect, Nitschke argues, scientists can begin to think about ways that knowledge could be used in clinical settings.

MRI and functional MRI in particular are turning out to be very powerful tools to aid our understanding of how we think. And yet, the techniques are still fairly crude, and haven't been used for long. I think many surprising and useful insights will be gained into many aspects of human behaviour and cognition within the next few years, that may well revolutionise our understanding of the nature of Human Intelligence.

About Me

Actually, I am a Rocket Scientist.
Also hormonally odd (my blood has 46xy chromosomes anyway) and for most of my life, I looked male, and lived as one, trying to be the best Man a Gal could be. Anyway, in May 2005 that started changing naturally for reasons still unclear, and I'm now Zoe, not Alan : happier and more relaxed not to have to pretend any more.
UPDATE - reason now identified as the 3BHSD form of CAH.

Reviews

This blog, written by a rocket scientist, is a fascinating collection of information, both personal and scientific, regarding intersex, transsexualism and related psychosocial and psychosexual issues....It is erudite and heartfelt. Just read the posts about the passport issue. You won't know whether to laugh, weep or crawl into a ball and rock gently in a corner - an amazing person.- David---The reason I so appreciate bright, perceptive people - as opposed to ideologues whose intelligence does little to illuminate - is that they manage to both instruct and learn with a certain grace. Among such rarities in the transblogosphere is Zoe, whose direct speech and clear humanity always make her worth reading, even if one doesn’t always agree with her every conclusion.- Val---The following is a request for permission to archive your A.E.Brain blog site which we have wanted to do for several years...The Library has traditionally collected items in print, but it is also committed to preserving electronic publications of lasting cultural value....Since (1996) we have been identifying online publications and archiving those that we consider have national significance....We would like to include A.E.Brain blog site in the PANDORA Archive...-Australian National Library